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体内小鼠皮肤中DNA加合物的32P后标记检测与一系列油产品中多环芳烃化合物含量及鼠伤寒沙门氏菌致突变性的相关性。

Correlation of 32P-postlabelling-detection of DNA adducts in mouse skin in vivo with the polycyclic aromatic compound content and mutagenicity in Salmonella typhimurium of a range of oil products.

作者信息

Booth E D, Brandt H C, Loose R W, Watson W P

机构信息

Toxicology Department, Shell International Chemicals B.V., Shell Research and Technology Centre Amsterdam, The Netherlands.

出版信息

Arch Toxicol. 1998 Jul-Aug;72(8):505-13. doi: 10.1007/s002040050535.

Abstract

The in vivo genotoxic activities in mouse skin of the dimethyl sulphoxide (DMSO) extracts of a range of oil products [residual aromatic extract; untreated heavy paraffinic distillate aromatic extract; mildly refined light naphthenic base oil; bitumen (vacuum residue); high viscosity index base oil obtained by catalytic hydrogenation] were evaluated by 32P-postlabelling DNA analysis. The results of quantitative 32P-postlabelling analyses of epidermal DNA from mice treated with the DMSO extracts showed linear relationships with the total polycyclic aromatic compound (PAC) contents, determined by the Institute of Petroleum method IP 346 and also the 3-6 ring PAC contents, measured by on-line liquid-liquid extraction using flow injection analysis. The 32P-postlabelling data also showed a linear relationship with the mutagenicity indices of these oil products determined in S. typhimurium TA98 using the modified Ames Salmonella microsome test. The in vivo genotoxicity of the DMSO extracts from the oil products was low, judged by 32P-postlabelling analysis of DNA adducts measured in epidermal DNA of treated mouse skin, and ranging from 2 to 723 attomole/microg DNA per mg oil product. The in vivo 32P-postlabelling data from this study are consistent with these materials expressing low genotoxicity in mouse skin in vivo. The DMSO extraction procedure coupled with 32P-postlabelling DNA analysis is useful for ranking the relative genotoxic potency in vivo of a wide range of oil products. In general the trend observed is similar to rankings based on physicochemical measurements of total PAC contents or 3 6 ring PAC contents of the oil products.

摘要

通过³²P后标记DNA分析,评估了一系列油品[残余芳烃提取物;未处理的重质石蜡馏分芳烃提取物;轻度精制的轻质环烷基基础油;沥青(减压渣油);催化加氢制得的高粘度指数基础油]的二甲基亚砜(DMSO)提取物在小鼠皮肤中的体内遗传毒性活性。用DMSO提取物处理的小鼠表皮DNA的³²P后标记定量分析结果,与采用石油学会方法IP 346测定的总多环芳烃化合物(PAC)含量以及采用流动注射分析在线液液萃取法测定的3 - 6环PAC含量呈线性关系。³²P后标记数据还与这些油品在鼠伤寒沙门氏菌TA98中采用改良的埃姆斯沙门氏菌微粒体试验测定的致突变性指数呈线性关系。根据对处理过的小鼠皮肤表皮DNA中DNA加合物的³²P后标记分析判断,油品的DMSO提取物的体内遗传毒性较低,范围为每毫克油品2至723阿托摩尔/微克DNA。本研究的体内³²P后标记数据与这些物质在小鼠皮肤体内表现出低遗传毒性一致。DMSO提取程序与³²P后标记DNA分析相结合,可用于对多种油品的体内相对遗传毒性效力进行排名。一般观察到的趋势与基于油品总PAC含量或3 - 6环PAC含量的物理化学测量的排名相似。

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